JP5956992B2 - Squalamine ophthalmic formulation - Google Patents
Squalamine ophthalmic formulation Download PDFInfo
- Publication number
- JP5956992B2 JP5956992B2 JP2013524928A JP2013524928A JP5956992B2 JP 5956992 B2 JP5956992 B2 JP 5956992B2 JP 2013524928 A JP2013524928 A JP 2013524928A JP 2013524928 A JP2013524928 A JP 2013524928A JP 5956992 B2 JP5956992 B2 JP 5956992B2
- Authority
- JP
- Japan
- Prior art keywords
- squalamine
- pharmaceutical composition
- ophthalmic
- ocular
- formulation
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Expired - Fee Related
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- AWDRATDZQPNJFN-VAYUFCLWSA-N taurodeoxycholic acid Chemical compound C([C@H]1CC2)[C@H](O)CC[C@]1(C)[C@@H]1[C@@H]2[C@@H]2CC[C@H]([C@@H](CCC(=O)NCCS(O)(=O)=O)C)[C@@]2(C)[C@@H](O)C1 AWDRATDZQPNJFN-VAYUFCLWSA-N 0.000 description 1
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- UEUXEKPTXMALOB-UHFFFAOYSA-J tetrasodium;2-[2-[bis(carboxylatomethyl)amino]ethyl-(carboxylatomethyl)amino]acetate Chemical compound [Na+].[Na+].[Na+].[Na+].[O-]C(=O)CN(CC([O-])=O)CCN(CC([O-])=O)CC([O-])=O UEUXEKPTXMALOB-UHFFFAOYSA-J 0.000 description 1
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Description
(関連出願の相互参照)
この出願は、米国特許第5,192,756(1993年3月9日に発行)、米国特許第6,962,909(2005年11月8日に発行)および米国特許第7,981,876(2011年7月19日)と技術的に関係しており、その全てを参照により本明細書に組み込む。
(Cross-reference of related applications)
No. 5,192,756 (issued on Mar. 9, 1993), U.S. Patent No. 6,962,909 (issued on Nov. 8, 2005) and U.S. Patent No. 7,981,876. (July 19, 2011), all of which are incorporated herein by reference.
(発明の分野)
本発明は、眼の症状、例えばウェット型加齢性黄斑変性症(ウェット型AMD)、脈絡膜血管新生、網膜症、ドライ型加齢性黄斑変性症(ドライ型AMD)、ポリープ状脈絡膜血管症、眼科手術後の血管新生、黄斑浮腫、網膜静脈閉塞症、下脈絡膜血管新生、網膜上皮剥離、翼状片または網膜色素上皮の中央窩地図状萎縮などの処置のための、スクアラミンまたはその医薬上許容し得る塩の眼用製剤に関する。
(Field of Invention)
The present invention relates to ocular symptoms such as wet age-related macular degeneration (wet AMD), choroidal neovascularization, retinopathy, dry age-related macular degeneration (dry AMD), polypoidal choroidal angiopathy, Squalamine or its pharmaceutically acceptable drugs for treatments such as angiogenesis after ophthalmic surgery, macular edema, retinal vein occlusion, hypochoroidal neovascularization, retinal epithelial detachment, pterygium or retinal pigment epithelium foveal map atrophy It relates to an ophthalmic formulation of the resulting salt.
(発明の背景)
加齢性黄斑変性症(AMD)は、アメリカ合衆国の中で52歳またはそれ以上の年齢の人々の中で不可逆的な中心視力損失の主要病因であり、アメリカ合衆国、カナダ、英国およびオーストラリアにおける失明の最も一般的な総合的原因である。AMDは、罹患患者の黄斑にて進行する幾つかの異常症状を含む。黄斑変性症には2つの形態が存在する:ドライ型(萎縮型としても知られる)およびウェット型(円盤状、滲出性、網膜下血管新生または脈絡膜血管新生としても知られる)。ウェット型の前兆ともいえるこのドライ型は、網膜により生成した不要物質を排出する黄斑色素上皮の能力欠損により生じる。ウェット型は、新しい血管が網膜下、特に黄斑で成長する場合におこる。
(Background of the Invention)
Age-related macular degeneration (AMD) is the leading cause of irreversible central vision loss among people aged 52 and older in the United States and is the most common cause of blindness in the United States, Canada, the United Kingdom, and Australia. It is a general general cause. AMD includes several abnormal symptoms that progress in the macular of affected patients. There are two forms of macular degeneration: dry (also known as atrophic) and wet (also known as discoid, exudative, subretinal neovascularization or choroidal neovascularization). This dry type, which is a precursor of the wet type, is caused by a defect in the ability of the macular pigment epithelium to discharge unwanted substances generated by the retina. The wet type occurs when new blood vessels grow under the retina, especially in the macula.
スクアラミン(IUPAC名:([6-[(3S,5R,7R,10S,13R,4S)-3-[3-(4-アミノブチルアミノ)プロピルアミノ]-7-ヒドロキシ-10,13-ジメチル-2,3,4,5,6,7,8,9,11,12,14,15,16,17-テトラデカヒドロ-1H-シクロペンタ[a]フェナントレン-17-イル]-2-メチルヘプタン-3-イル]硫酸水素塩)は、抗血管形成特性を示すアミノステロールであって、疾患の進行を特徴づける網膜における新血管形成および血管形成異常を防止するように働くウェット型AMDの効果的処置のための静脈内点滴として用いられている(Sills Jr. et al., "Squalamine Inhibits Angiogenesis and Solid Tumor Growth in Vivo Perturbs Embyronic Vasculature", Jul. 1, 1998, Cancer Research, 58, 2784-2792;Higgins et al., "Squalamine Improves Retinal Neovascularization", May 2000, Investigative Ophthalmology & Visual Science, vol. 41, No. 6, pp. 1507-1512.;PRNEWSWIRE, "Genaera Reports Squalamine Continues to Improve Vision at Four Months Timepoint in Age-Related Macular Degeneration",Oct. 7, 2003, http://www.eyesightnews.com/topic/28.html.)。スクアラミンは、Zasloffらの米国特許第5,192,756の主題であり、その全ては出典明示により本明細書に組み込まれる。スクアラミンの全体の化学合成は、米国特許第6,262,283および6,610,866に記述されており、その全ては出典明示により本明細書に組み込まれる。 Squalamine (IUPAC name: ([6-[(3S, 5R, 7R, 10S, 13R, 4S) -3- [3- (4-aminobutylamino) propylamino] -7-hydroxy-10,13-dimethyl- 2,3,4,5,6,7,8,9,11,12,14,15,16,17-tetradecahydro-1H-cyclopenta [a] phenanthren-17-yl] -2-methylheptane- 3-yl] bisulfate) is an aminosterol that exhibits anti-angiogenic properties and is an effective treatment for wet AMD that acts to prevent neovascularization and angiogenesis abnormalities in the retina that characterize disease progression (Sills Jr. et al., "Squalamine Inhibits Angiogenesis and Solid Tumor Growth in Vivo Perturbs Embyronic Vasculature", Jul. 1, 1998, Cancer Research , 58, 2784-2792; Higgins et al., "Squalamine Improves Retinal Neovascularization", May 2000, Investigative Ophthalmology & Visual Science , vol. 41, No. 6, pp. 1507-1512.; PRNEWSWIRE, "Genaera Reports Squalamine Continues to Improve Vision at Four Months Timepoint in Age-Related Macular Degeneration", Oct. 7, 2003, http: //www.eyesightnews .com / topic / 28.html.). squalamine is the U.S. Patent No. 5,192,756 of the subject Zasloff et al, all of which are incorporated herein by reference. total chemical synthesis of squalamine US Pat. Nos. 6,262,283 and 6,610,866, all of which are incorporated herein by reference.
患者の使用およびリスク的見地より、静脈内点滴、あるいは特に眼への直接的な注射を月に一度必要とする現行の治療標準とは異なり、眼に直接適用するために利用できる局所製剤が強く望まれる。医療施術管理下での高価な施与が必要であり、かつ眼内炎および網膜剥離などの重篤な合併症をもたらす可能性がある侵襲性が高い技術(例えば、静脈内点滴)と比べて、局所製剤(例えば、溶液、懸濁、クリームまたは軟膏などの形態にある製剤)は、患者による自主投与が容易である。しかし、眼用点眼薬が持つ一般的な問題とは、その投与後に、通常点眼薬中の薬剤成分の5%未満が、角膜を透過して、眼球内組織に到達することである。その代わりに、投与用量の主要部は、溶液排出および全身吸収により排除される(Jarvinen K. et al., "Ocular absorption following topical delivery", Adv. Drug Deliv. Rev. 1995; 16(1):3-19. See also Conroy C.W., "Sulfonamides do not reach the retina in therapeutic amounts after topical application to the cornea", Ocul. Pharmacol. Ther. 1997; 13(5):465-472 and Maurice D.M., "Drug delivery to the posterior segment from drops", Surv. Ophthalmol. 2002;47(suppl. 1):S41-S52)。 Unlike current treatment standards that require intravenous infusion, or especially direct eye injection once a month, the topical formulation available for direct application to the eye is strong due to patient use and risk considerations. desired. Compared to highly invasive techniques (eg, intravenous infusion) that require expensive administration under medical care management and can cause serious complications such as endophthalmitis and retinal detachment Topical formulations (eg, formulations in the form of solutions, suspensions, creams or ointments, etc.) are easy to administer by the patient. However, a general problem with ophthalmic eye drops is that, after administration, less than 5% of the drug component in normal eye drops penetrates the cornea and reaches the intraocular tissue. Instead, the main part of the administered dose is eliminated by solution excretion and systemic absorption (Jarvinen K. et al., “Ocular absorption following topical delivery”, Adv. Drug Deliv. Rev. 1995; 16 (1): 3-19. See also Conroy CW, "Sulfonamides do not reach the retina in therapeutic amounts after topical application to the cornea", Ocul. Pharmacol. Ther. 1997; 13 (5): 465-472 and Maurice DM, "Drug delivery to the posterior segment from drops ", Surv. Ophthalmol. 2002; 47 (suppl. 1): S41-S52).
さらに、IV点滴によるAMD処置に対するスクアラミンの効力を試験する先の臨床試験により、長期的使用についての潜在的問題が明らかとなった。IV製剤での静脈投薬療法は、薬物動態分析を用いると最適以下であると見なされ、様々な理由により商業規模では利用できなかった。一例として、40mgの投薬時のヒト対象中のスクアラミンの短期血漿半減期は、4〜6日後には脈絡膜血管新生(CNV)を防止するためには不十分な脈絡膜中の濃度となる。月に1回の"維持"点滴に対してこの投薬を忘れた場合、わずか一週まではCNVを阻害できるが、その後3週間に活発な新規血管新生がおこる可能性がある。この治療方法は、投与最初の4〜5週間後に視力の良好な回復をもたらし、その後の第5週後に改善率の低下をもたらした。静脈内投薬は、局所輸注反応を引き起こした(投薬は、局所製剤に使用される投薬量よりも非常に多い)。「現実社会」の状況下では、ウェット型AMDの高齢患者が長時間の点滴のために週一回の頻度で来院できると期待することは非現実である。殆どの網膜の眼用処置は、このような静脈内点滴としても設定されていない。 Furthermore, previous clinical trials examining the efficacy of squalamine for AMD treatment by IV infusion revealed potential problems for long-term use. Intravenous medication with IV formulations was considered suboptimal using pharmacokinetic analysis and was not available on a commercial scale for a variety of reasons. As an example, the short plasma half-life of squalamine in a human subject at a dose of 40 mg results in a concentration in the choroid that is insufficient to prevent choroidal neovascularization (CNV) after 4-6 days. If this medication is forgotten for a monthly "maintenance" infusion, CNV can be inhibited for up to a week, but active neovascularization may occur in the next 3 weeks. This treatment method resulted in a good recovery of visual acuity after the first 4-5 weeks of administration and a reduction in improvement after the fifth week thereafter. Intravenous dosing caused a local infusion response (dosing was much higher than the dosage used for topical formulations). Under the “real world” situation, it is unrealistic to expect wet AMD elderly patients to visit once a week for long infusions. Most retinal ophthalmic procedures are not set up as such intravenous infusions.
本発明は、静脈内投薬に関連がある上記欠点と比べて、疾患を処置するための、眼の後部に治療薬の選択的送達を達成できる局所投与用の安全かつ非刺激性の眼用製剤の発見を示すものである。 The present invention provides a safe and non-irritating ophthalmic formulation for topical administration that can achieve selective delivery of a therapeutic agent to the back of the eye to treat disease compared to the above-mentioned drawbacks associated with intravenous dosing This indicates the discovery.
(発明の要旨)
本発明の一態様は、スクアラミンまたはその医薬上許容し得る塩、1以上の粘膜接着剤および1以上の浸透増強剤を含む、局所用の眼用用途のための組成物である。
(Summary of the Invention)
One aspect of the present invention is a composition for topical ophthalmic use comprising squalamine or a pharmaceutically acceptable salt thereof, one or more mucoadhesive agents and one or more penetration enhancers.
本発明の別の態様において、該組成物は、さらに増粘剤、張度改変剤、抗菌性防腐剤、緩衝剤、界面活性剤、安定化剤、可溶化剤および再懸濁剤の少なくとも一つを含む。 In another embodiment of the present invention, the composition further comprises at least one of a thickener, a tonicity modifier, an antibacterial preservative, a buffer, a surfactant, a stabilizer, a solubilizer and a resuspending agent. Including one.
本発明の別の態様は、眼症状の予防および/または処置が必要なヒトなどの哺乳動物の眼に、治療上有効量のスクアラミンまたはその医薬上許容し得る塩を、局所投与することを含む、眼症状を予防および/または処置するための方法である。 Another aspect of the present invention involves topical administration of a therapeutically effective amount of squalamine or a pharmaceutically acceptable salt thereof to the eyes of a mammal, such as a human, in need of prevention and / or treatment of ocular symptoms. A method for preventing and / or treating ocular symptoms.
例示的な実施形態において、該眼症状は、ウェット型加齢性黄斑変性症(ウェット型AMD)、脈絡膜血管新生、網膜症またはドライ型加齢性黄斑変性症(ドライ型AMD)および網膜色素上皮の中央窩地図状萎縮からなる群から選択される。 In exemplary embodiments, the ocular symptoms are wet age-related macular degeneration (wet AMD), choroidal neovascularization, retinopathy or dry age-related macular degeneration (dry AMD) and retinal pigment epithelium. Selected from the group consisting of:
例示的な実施形態において、スクアラミンは、そのジラクテート塩として存在する。 In an exemplary embodiment, squalamine is present as its dilactate salt.
例示的な実施形態において、該組成物は、さらに非イオン性張度改変剤、塩、防腐剤、緩衝剤、界面活性剤、可溶化剤および安定化剤の少なくとも一つを含む。 In an exemplary embodiment, the composition further comprises at least one of a nonionic tonicity modifier, a salt, a preservative, a buffer, a surfactant, a solubilizer, and a stabilizer.
例示的な実施形態において、該組成物は局所投与される。 In an exemplary embodiment, the composition is administered topically.
例示的な実施形態において、該組成物は、点眼薬、ゲル、ローション、クリーム、軟膏の形態にて存在しており、薬剤溶出眼用コンフォーマー、侵食性インプラント、強膜近傍(juxtascleral)インプラント、涙管ステント、イオントフォレーシス眼送達系または眼用スプレー薬剤送達デバイスに組み込まれる。 In an exemplary embodiment, the composition is present in the form of eye drops, gels, lotions, creams, ointments, drug eluting ophthalmic conformers, erodible implants, juxtascleral implants, Incorporated into lacrimal stents, iontophoretic ocular delivery systems or ophthalmic spray drug delivery devices.
本発明の態様は、スクアラミンまたはその医薬上許容し得る塩;1以上の粘膜接着剤;および1以上の浸透増強剤を含む組成物を投与することにより、哺乳動物の眼の後部強膜にスクアラミンまたはその医薬上許容し得る塩を治療上有効量にて送達し、同時に房水または硝子体液中に該組成物の無視できる濃度をもたらす、方法である。 Embodiments of the present invention include squalamine in the posterior sclera of a mammalian eye by administering a composition comprising squalamine or a pharmaceutically acceptable salt thereof; one or more mucoadhesives; and one or more penetration enhancers. Or a method wherein a pharmaceutically acceptable salt thereof is delivered in a therapeutically effective amount, while at the same time providing a negligible concentration of the composition in the aqueous humor or vitreous humor.
例示的な実施形態において、粘膜接着剤は、カルボポール980、ヒドロキシプロピルメチルセルロース、ポビドンK-30およびポリビニルアルコールからなる群から選択される。 In an exemplary embodiment, the mucoadhesive agent is selected from the group consisting of carbopol 980, hydroxypropylmethylcellulose, povidone K-30 and polyvinyl alcohol.
例示的な実施形態において、浸透増強剤は、n-ドデシル-β-D-マルトシド、ラウロカプラムおよびグリセロールモノラウレート、およびPGML(ポリエチレングリコールモノラウレート)からなる群から選択される。 In an exemplary embodiment, the penetration enhancer is selected from the group consisting of n-dodecyl-β-D-maltoside, laurocapram and glycerol monolaurate, and PGML (polyethylene glycol monolaurate).
例示的な実施形態において、眼症状はウェット型AMDである。 In an exemplary embodiment, the ocular condition is wet AMD.
例示的な実施形態において、スクアラミンジラクテートは、0.005〜5.0重量%の量で存在する。 In an exemplary embodiment, squalamine dilactate is present in an amount of 0.005 to 5.0% by weight.
例示的な実施形態において、非イオン性張度改変剤は、約50〜350ミリオスモル/kgの張度とするために十分な量で存在する。 In an exemplary embodiment, the nonionic tonicity modifying agent is present in an amount sufficient to achieve a tonicity of about 50 to 350 milliosmol / kg.
例示的な実施形態において、該塩は、ヒトの涙の塩濃度および/または張度に近づけるために十分な量で存在する。 In an exemplary embodiment, the salt is present in an amount sufficient to approximate human tear salt concentration and / or tonicity.
例示的な実施形態において、該塩は、0.3%〜1重量%の範囲の量で存在する。 In an exemplary embodiment, the salt is present in an amount ranging from 0.3% to 1% by weight.
例示的な実施形態において、該防腐剤は、約12時間〜約72時間の間、微生物濃度を維持または減少させるための微生物バリアを生み出すのに十分な量で存在する。 In an exemplary embodiment, the preservative is present in an amount sufficient to create a microbial barrier to maintain or reduce microbial concentration for between about 12 hours and about 72 hours.
図は、本発明の範囲の単に代表的実施形態を示すものであり、本発明の範囲を別途制限するものではない。 The figures merely illustrate exemplary embodiments of the scope of the invention and do not limit the scope of the invention separately.
(発明の詳細な説明)
例示的な実施形態において、本発明の眼用製剤は、スクアラミンまたはその医薬上許容し得る塩、粘膜接着剤および浸透増強剤を含有する。該製剤は、所望により以下の少なくとも1つの成分を含むが、これに限定するものではない:(a)張度改変剤;(b)抗菌性防腐剤;(c)緩衝剤;(d)界面活性剤;(e)安定化剤;(f)可溶化剤または再懸濁剤;(g)別の粘膜接着剤;および(h)別の浸透増強剤。
(Detailed description of the invention)
In an exemplary embodiment, the ophthalmic formulation of the present invention contains squalamine or a pharmaceutically acceptable salt thereof, a mucoadhesive agent and a penetration enhancer. The formulation optionally includes, but is not limited to, at least one of the following components: (a) a tonicity modifying agent; (b) an antimicrobial preservative; (c) a buffering agent; (d) an interface. (E) a stabilizer; (f) a solubilizer or resuspension agent; (g) another mucoadhesive; and (h) another penetration enhancer.
本発明の局所製剤は、眼の後部を標的とすると考えられる。眼の後部を標的とする際に有利である局所製剤として、それは十分な濃度で眼の後部強膜に到達できる特性を有するべきである。理想としては、該製剤は、眼の背面へ、例えば、前方強膜から後部強膜へ拡散する前に涙で流されずに角膜上での滞留時間を増加すべきである。薬剤分子が眼の水晶体に悪影響を及ぼすかも知れないので(例えば、水晶体混濁により)、該薬剤分子は眼の前面から球体内を通過して、任意の相当量まで眼球内の房水および硝子体液へ入るべきではない。本発明の製剤は、眼の前面に適用される薬剤分子、例えばスクアラミンまたはその医薬上許容し得る塩を、薬剤分子の治療濃度が目的とする疾患の処置に必要とされる眼の後面に有効に送達するために必要とされる所望のかつ独特な特徴を有している。眼の表面上に投与した後に、該組成物は、結膜および前方強膜に入り、角膜層に入る。粘膜接着剤は、薬剤が後部強膜まで時間をかけてゆっくりと拡散できるように角膜中の滞留時間を増加させて、後部強膜中のスクアラミンまたはその医薬上許容し得る塩濃度の徐放性送達をもたらすと考えられる。該粘膜接着剤は、該薬剤の損失、例えば鼻涙管からの排出、流涙および涙のターンオーバーを遅延させることによりこの目的を達成する。また、該粘膜接着剤は、一般的に所望の鎮静または潤滑効果をもたらすことができる粘度増強特性を有する。該製剤に所望により添加してもよい浸透増強剤は、角膜上皮層への該製剤の浸透性を増強して、眼内のスクアラミンまたはその医薬上許容し得る塩の滞留時間をさらに増強する。該安定化剤は、抗酸化剤として作用し得るか、またはスクアラミン製剤の化学的分解を遅延させ得る。該緩衝剤は、該製剤を眼投与に適合し得る安定なほぼ中性pHに緩衝する。該製剤中の張度改変剤は、眼用製剤の適切な張度を提供する。 The topical formulations of the present invention are believed to target the back of the eye. As a topical formulation that is advantageous in targeting the posterior part of the eye, it should have the property of reaching the posterior sclera of the eye at a sufficient concentration. Ideally, the formulation should increase the residence time on the cornea without being shed by tears before diffusing to the back of the eye, eg, from the anterior sclera to the posterior sclera. Since drug molecules may adversely affect the lens of the eye (eg, due to lens opacity), the drug molecules pass through the sphere from the front of the eye to any substantial amount in the aqueous humor and vitreous humor in the eye Should not enter. The formulations of the present invention effectively apply a drug molecule applied to the front of the eye, such as squalamine or a pharmaceutically acceptable salt thereof, to the posterior surface of the eye where a therapeutic concentration of the drug molecule is required for the treatment of the target disease. It has the desired and unique characteristics needed to deliver it. After administration on the surface of the eye, the composition enters the conjunctiva and anterior sclera and enters the corneal layer. Mucoadhesives increase the residence time in the cornea so that the drug slowly diffuses over time to the posterior sclera, allowing sustained release of squalamine or its pharmaceutically acceptable salt concentration in the posterior sclera. It is thought to result in delivery. The mucoadhesive achieves this goal by delaying the loss of the drug, such as drainage from the nasolacrimal duct, lacrimation and tear turnover. The mucoadhesives also generally have viscosity enhancing properties that can provide the desired soothing or lubricating effect. A penetration enhancer that may optionally be added to the formulation enhances the penetration of the formulation into the corneal epithelial layer and further enhances the residence time of squalamine or a pharmaceutically acceptable salt thereof in the eye. The stabilizer may act as an antioxidant or delay chemical degradation of the squalamine formulation. The buffering agent buffers the formulation to a stable near neutral pH that is compatible with ocular administration. The tonicity modifying agent in the formulation provides the appropriate tonicity of the ophthalmic formulation.
得られる製剤は安定であって、滅菌後に梱包されても、貯蔵されても、直接使用されてもよい。例示的な実施形態において、該製剤は、点眼薬とするために通常使用される様式の液滴形態で存在しうる。通常のスクイーズ型の液滴適用装置は、本発明の眼用製剤を適用する際に使用するために非常に好適である。例示的な実施形態において、該製剤は、使用者の罹患眼(複数含む)へ該製剤の液滴を添加することにより便宜的に投与される。 The resulting formulation is stable and may be packaged after sterilization, stored, or used directly. In an exemplary embodiment, the formulation may be in the form of droplets in the manner commonly used to make eye drops. A normal squeeze-type droplet application device is very suitable for use in applying the ophthalmic preparation of the present invention. In an exemplary embodiment, the formulation is conveniently administered by adding droplets of the formulation to the user's affected eye (s).
防腐剤を含有する本発明の製剤は、多回投与用容器における使用に特に有利である。本明細書で使用した多回投与用容器は、該容器内に存在する眼用製剤を2回以上別々に適用できる容器をいう。かかる容器は、再封入可能である−即ち、該容器キャップは、最初の適用のために取り外すことができ、その後該キャップを該容器上で再置することにより、実質的な液体の不浸透性密閉を再度提供できる。例示的な実施形態において、抗菌性防腐剤は、約12時間〜約72時間、例えば約12時間〜約48時間、例えば約12時間〜約24時間の間、微生物濃度を減少させるために十分な量で存在する。 The formulations of the invention containing preservatives are particularly advantageous for use in multi-dose containers. As used herein, a multi-dose container refers to a container to which the ophthalmic preparation present in the container can be separately applied two or more times. Such containers can be re-enclosed--i.e., The container cap can be removed for initial application, and then the liquid can be substantially impervious by repositioning the cap over the container. Sealing can be provided again. In an exemplary embodiment, the antimicrobial preservative is sufficient to reduce the microbial concentration for between about 12 hours to about 72 hours, such as between about 12 hours to about 48 hours, such as between about 12 hours to about 24 hours. Present in quantity.
例示的な実施形態において、防腐剤を含有しないそれらの製剤は、単回用量容器に梱包される―即ち、単回用量が所定の容器により提供できる場合。かかる防腐剤不含組成物は、使用者が一旦該容器の密封を破ると、制御できない微生物増殖に付される。そのため、使用者は、最初の投与後に該容器の廃棄が指示される。好適な単位用量系、例えば成型同時充填(blow-fill-seal)単位用量の防腐剤不含梱包システムは、防腐剤不含製剤のために一般的に使用される。 In an exemplary embodiment, those formulations that do not contain preservatives are packaged in a single dose container—ie, where a single dose can be provided by a given container. Such preservative-free compositions are subject to uncontrolled microbial growth once a user breaks the seal of the container. Thus, the user is instructed to discard the container after the first dose. Suitable unit dose systems such as blow-fill-seal unit dose preservative-free packaging systems are commonly used for preservative-free formulations.
本発明のスクアラミンまたはその塩の局所眼用投与のための医薬組成物は、従来の眼科的に適合し得る賦形剤、例えば軟膏、クリーム、懸濁液、ローション、粉末、溶液、ペースト、ゲル、スプレー、エアゾールまたは油の中に製剤され得る。 The pharmaceutical composition for topical ophthalmic administration of squalamine or a salt thereof of the present invention comprises conventional ophthalmically compatible excipients such as ointments, creams, suspensions, lotions, powders, solutions, pastes, gels. Can be formulated in sprays, aerosols or oils.
本明細書で使用されたとおりに、用語"黄斑変性症"は、黄斑変性症の全ての形態を包含し、高齢者にて特に発症する片眼または両眼に通常影響を及ぼす中心視力の段階的損失を含むことが意図される。通常ドライ型といわれる黄斑変性症のゆっくりとした進行形態は、特に網膜の黄色沈着物の蓄積および網膜の薄化を特徴とする。通常ウェット型としていわれる黄斑変性症の急速な進行形態は、出血を示す痕跡化および網膜下で形成された新規血管からの液体漏出を特徴とする。黄斑変性症は、ウェット型またはドライ型のいずれかとして存在し得る。 As used herein, the term “macular degeneration” encompasses all forms of macular degeneration, a stage of central vision that usually affects one or both eyes, especially in older people It is intended to include technical losses. The slowly progressive form of macular degeneration, usually referred to as dry, is particularly characterized by the accumulation of yellow deposits of the retina and thinning of the retina. The rapidly progressive form of macular degeneration, usually referred to as wet, is characterized by evidence of bleeding and fluid leakage from new blood vessels formed under the retina. Macular degeneration can exist as either wet or dry type.
本明細書に規定されるとおり、"治療上有効量"とは、全体的または部分的に症状の進行を阻害するか、または少なくとも部分的に1以上の症状の徴候を緩和する有効成分(例えば、スクアラミン)の量である。治療上有効量は、予防的に有効な量でもあり得る。治療上有効である量は、患者の大きさ、性別、処置される症状、症状の重症度および目的とする結果に依存する。所定の患者について、治療上有効量を、当業者には既知の方法により決定する。スクアラミンまたはその医薬上許容し得る塩の濃度は、通常、約0.005〜約5.0重量%、例えば約0.010〜約4.0重量%、例えば約0.020〜約3.0重量%、例えば約0.030〜約2.0重量%、例えば約0.050〜約1.0重量%で存在し得る。 As defined herein, a “therapeutically effective amount” is an active ingredient that inhibits, in whole or in part, the progression of symptoms, or at least partially alleviates one or more symptoms of symptoms (eg, , Squalamine). A therapeutically effective amount can also be a prophylactically effective amount. The amount that is therapeutically effective depends on the size, sex, symptom being treated, severity of symptoms and the desired outcome. For a given patient, the therapeutically effective amount is determined by methods known to those skilled in the art. The concentration of squalamine or a pharmaceutically acceptable salt thereof is typically about 0.005 to about 5.0% by weight, such as about 0.010 to about 4.0% by weight, such as about 0.020 to about 3.0. It may be present in weight percent, such as about 0.030 to about 2.0 weight percent, such as about 0.050 to about 1.0 weight percent.
例示的な実施形態において、該スクアラミンは、ジラクテート塩の形態である。例示的な実施形態において、スクアラミンジラクテート塩を、約0.1〜約0.3% w/v、例えば約0.1〜0.2% w/vの濃度で用いる。 In an exemplary embodiment, the squalamine is in the form of a dilactate salt. In an exemplary embodiment, squalamine dilactate salt is used at a concentration of about 0.1 to about 0.3% w / v, such as about 0.1 to 0.2% w / v.
所望により、本発明の製剤は、張度改変剤を含有する。例示的な実施形態において、該張度改変剤が非イオン性である。該張度改変剤は、次のものから選択され得るが、これらに限定するものではない:マンニトール、ソルビトール、デキストロース、精製白糖、尿素、グリセロール、ポリエチレングリコールおよびその任意の混合物。例示的な実施形態において、該張度改変剤は、約50〜約350 ミリオスモル/kg(mOsmol/kg)、例えば約65〜約325 mOsmol/kg、例えば約80〜約310 mOsmol/kg、例えば約95〜約295 mOsmol/kg、例えば約110〜約280 mOsmol/kg、例えば約125〜約265 mOsmol/kg、例えば約140〜約250 mOsmol/kg、例えば約155〜約235 mOsmol/kg、例えば約170〜約220 mOsmol/kg、例えば約185〜約205 mOsmol/kgの張度を生み出す十分な量で存在する。 If desired, the formulations of the present invention contain a tonicity modifying agent. In an exemplary embodiment, the tonicity modifying agent is nonionic. The tonicity modifying agent can be selected from, but not limited to: mannitol, sorbitol, dextrose, purified sucrose, urea, glycerol, polyethylene glycol and any mixture thereof. In an exemplary embodiment, the tonicity modifying agent is about 50 to about 350 milliosmol / kg (mOsmol / kg), such as about 65 to about 325 mOsmol / kg, such as about 80 to about 310 mOsmol / kg, such as about 95 to about 295 mOsmol / kg, such as about 110 to about 280 mOsmol / kg, such as about 125 to about 265 mOsmol / kg, such as about 140 to about 250 mOsmol / kg, such as about 155 to about 235 mOsmol / kg, such as about It is present in an amount sufficient to produce a tonicity of 170 to about 220 mOsmol / kg, such as about 185 to about 205 mOsmol / kg.
該製剤は、下記から選択されるイオン性塩を含有し得るが、これらに限定するものではない:約0.3〜約1重量%の量またはヒトの涙の塩濃度および/または張度に近づけるために十分な量のアルカリ金属ハライド(例えば、NaCl、KCl、NaBrなど)。この群からの選択された塩は、イオン性張度改変剤ともいえる。 The formulation may contain, but is not limited to, an ionic salt selected from: in an amount of about 0.3 to about 1% by weight or in human tear salt concentration and / or tonicity. A sufficient amount of alkali metal halide (eg, NaCl, KCl, NaBr, etc.) to approximate. Selected salts from this group can also be referred to as ionic tonicity modifiers.
防腐剤が本発明の製剤に使用される場合、殺菌剤は、微生物濃度を維持または減少させるために、約12時間〜約72時間、例えば約12時間〜約48時間、例えば約12時間〜約24時間の間、微生物バリアを生み出すのに十分な量で存在する。防腐剤には、次のものを含むが、これらに限定するものではない:塩化ベンザルコニウム、ベンジルアルコール、クロロブタノール、セトリモニウム、メチルパラベン、プロピルパラベン、ポリアミノプロピルビグアニド、フェニルエチルアルコール、クロロヘキシジン、クロロヘキシジンジグルコネート、クロロクワット、安定化オキシクロロ錯体またはその任意の組合せ。 When preservatives are used in the formulations of the present invention, the bactericidal agent is about 12 hours to about 72 hours, such as about 12 hours to about 48 hours, such as about 12 hours to about, to maintain or reduce the microbial concentration. It is present in an amount sufficient to create a microbial barrier for 24 hours. Preservatives include, but are not limited to: benzalkonium chloride, benzyl alcohol, chlorobutanol, cetrimonium, methyl paraben, propyl paraben, polyaminopropyl biguanide, phenylethyl alcohol, chlorohexidine, chloro Hexidine digluconate, chloroquat, stabilized oxychloro complex or any combination thereof.
本発明の製剤に使用され得る緩衝剤は、ナトリウム、炭酸水素カリウム、リン酸塩、酢酸塩、クエン酸塩、ホウ酸塩および/またはリン酸、酢酸、クエン酸またはホウ酸から調製された緩衝液を含むが、これらに限定されない。例示的な実施形態において、該緩衝液は、リン酸二水素ナトリウムまたはリン酸ナトリウムまたはホウ酸/ホウ酸ナトリウムである。本発明の緩衝液は、約5.5〜約8.0、例えば約5.7〜約7.7、例えば約6.0〜約7.4、例えば約6.3〜約7.1、例えば約6.6〜約6.8の生成物pH、または約5.7、約5.9、約6.1、約6.3、約6.5、約6.7、約6.9、約7.1、約7.3、約7.5、約7.7または約7.9のpHを維持するのに十分な量で存在すべきである。 Buffers that can be used in the formulations of the present invention are buffers prepared from sodium, potassium bicarbonate, phosphate, acetate, citrate, borate and / or phosphoric acid, acetic acid, citric acid or boric acid. Including but not limited to liquid. In an exemplary embodiment, the buffer is sodium dihydrogen phosphate or sodium phosphate or boric acid / sodium borate. The buffer of the present invention has a pH of about 5.5 to about 8.0, such as about 5.7 to about 7.7, such as about 6.0 to about 7.4, such as about 6.3 to about 7.1. For example, a product pH of about 6.6 to about 6.8, or about 5.7, about 5.9, about 6.1, about 6.3, about 6.5, about 6.7, about 6.9. Should be present in an amount sufficient to maintain a pH of about 7.1, about 7.3, about 7.5, about 7.7 or about 7.9.
界面活性剤もまた本発明の製剤に添加できる。例示的な実施形態において、該界面活性剤は、該製剤に対して増強された湿潤特性を提供するために、約0.001%〜約0.3%、例えば約0.005%〜約0.2%、例えば約0.01%〜約0.1%、例えば約0.05%〜約0.1%の濃度範囲で存在する。該界面活性剤は、次のものを含むが、これらに限定するものではない:ポロキサマー、ポリソルベート80、ポリソルベート20、チロキサポール、ポリオキソエチレン、Brij 35、Brij 58、Brij 78、Aptet 100、G1045、Spans 20、40および85、Tweens 20、40、80または81、ラウロイルサルコシンナトリウム、ラウロイル-L-グルタミン酸トリエタノールアミン、ミリストイルサルコシンナトリウムおよびラウリル硫酸ナトリウム、ポリオキシエチレンソルビタン脂肪酸エステル、ポリオキシエチレン水素化ヒマシ油、ポリエチレングリコール脂肪酸エステル(例えば、ステアリン酸ポリオキシル)、ポリオキシエチレンポリオキシプロピレンアルキルエーテル、ポリオキシアルキレンアルキルフェニルエーテル、ポリグリセリン脂肪酸エステル(例えば、デカグリセリルモノラウレート)、グリセロール脂肪酸エステル、ソルビタン脂肪酸エステルおよびポリオキシエチレンポリオキシプロピレングリコール(poloxamer)、デカグリセリルモノラウレート、ステアリン酸ポリオキシル40、およびポリオキシエチレン水素化ヒマシ油、またはその任意の組合せ。
Surfactants can also be added to the formulations of the present invention. In exemplary embodiments, the surfactant is from about 0.001% to about 0.3%, such as from about 0.005% to about 0, to provide enhanced wetting properties to the formulation. It is present in a concentration range of 0.2%, such as from about 0.01% to about 0.1%, such as from about 0.05% to about 0.1%. Such surfactants include, but are not limited to: poloxamer, polysorbate 80, polysorbate 20, tyloxapol, polyoxoethylene,
安定化剤もまた本発明の製剤に添加できる。好適な安定化剤には次のものを含むが、これらに限定するものではない:メタ重亜硫酸ナトリウム塩、硫酸水素ナトリウム、アセチルシステイン、アスコルビン酸、チオ硫酸ナトリウム、αトコフェロール、カルノシン、レチニル・パルミテート、エチレンジアミンテトラ酢酸塩(EDTA)(例えば、ジナトリウム、テトラナトリウム、カルシウムまたはカルシウムエデト酸ナトリウム)、またはその組合せ。 Stabilizers can also be added to the formulations of the present invention. Suitable stabilizers include, but are not limited to: sodium metabisulfite, sodium bisulfate, acetylcysteine, ascorbic acid, sodium thiosulfate, alpha tocopherol, carnosine, retinyl palmitate , Ethylenediaminetetraacetate (EDTA) (eg disodium, tetrasodium, calcium or sodium calcium edetate), or combinations thereof.
記述された製剤に存在する粘膜接着剤は、角膜接触時間を増加し、バイオアベイラビリティーを増強し、および/または潤滑効果を提供し、そして次のものを含むがこれらに限定されない:アクリル酸ポリマー、メチルセルロース、エチルセルロース、ヒドロキシプロピルメチルセルロース、ヒドロキシエチルセルロース、Carbopol(登録商標) ポリマー(例えば、Carbopol(登録商標)674、676、690、980 NF、ETD-2691、ETD 2623、EZ-2、EZ-3、EZ-4、Aqua 30およびNovethix(登録商標)L-10)、ヒドロキシプロピルセルロース、ポリビニルアルコール、酢酸セルロース、フタレート、アルギネート、ゼラチン、コンドロイチン硫酸ナトリウム、または任意のその組合せ。 The mucoadhesive present in the described formulation increases corneal contact time, enhances bioavailability, and / or provides a lubricating effect and includes, but is not limited to: acrylic acid polymer , Methylcellulose, ethylcellulose, hydroxypropylmethylcellulose, hydroxyethylcellulose, Carbopol (R) polymer (e.g. Carbopol (R) 674,676, 690, 980 NF, ETD-2661, ETD-2623, EZ-2, EZ-3, EZ-4, Aqua 30 and Novethix (TM) L-10), hydroxypropylcellulose, polyvinyl alcohol, cellulose acetate, phthalate, alginates, gelatin, sodium chondroitin sulfate, or any combination thereof,
記述された製剤に存在する浸透増強剤は、次のものを包含するが、これらに限定するものではない:ラウロカプラム(azone)、胆汁酸およびそのアルカリ金属塩、例えばケノデオキシコール酸、コール酸、タウロコール酸、タウロデオキシコール酸、タウロウルソデオキシコール酸またはウルソデオキシコール酸、グリココレート、n-ドデシル-β-D-マルトシド、シュクロースドデカノエート、オクチルマルトシド、デシルマルトシド、トリデシルマルトシド、テトラデシルマルチドシド、ヘキサメチレンラウラミド、ヘキサメチレンオクタンアミド、グリセロールモノラウレート、PGML(ポリエチレングリコールモノラウレート)、ジメチルスルホキシド、メチルスルホニルメタン、フシジン酸ナトリウム、サポニンまたはその任意の組合せなど。 Penetration enhancers present in the described formulations include, but are not limited to: laurocapram, bile acids and alkali metal salts thereof such as chenodeoxycholic acid, cholic acid, taurocholic acid , Taurodeoxycholic acid, tauroursodeoxycholic acid or ursodeoxycholic acid, glycocholate, n-dodecyl-β-D-maltoside, sucrose dodecanoate, octyl maltoside, decyl maltoside, tridecyl maltoside, tetra Decyl malidoside, hexamethylene lauramide, hexamethylene octanamide, glycerol monolaurate, PGML (polyethylene glycol monolaurate), dimethyl sulfoxide, methylsulfonylmethane, sodium fusidate, saponin or any combination thereof Etc..
さらに、可溶化剤または再懸濁剤を、本発明の製剤に添加してもよい。好適な可溶化剤または再懸濁剤には、次のものを包含するが、これらに限定するものではない:シクロデキストリン(CD)、例えばヒドロキシプロピルγ-CD(Cavasol(登録商標))、スルホブチルエーテル4β-CD(Captisol(登録商標))およびヒドロキシプロピルβ-CD(Kleptose(登録商標))、ポリソルベート80(Tween80(登録商標))またはヒアルロン酸またはヒアルロン酸塩。該シクロデキストリンは、特に透過増強特性も示し得る。 In addition, solubilizers or resuspensions may be added to the formulations of the present invention. Suitable solubilizing agents or re-suspending agents, encompasses the following: and are not limited to: cyclodextrin (CD), such as hydroxypropyl γ-CD (Cavasol (R)), sulfo ether 4β-CD (Captisol (R)) and hydroxypropylmethylcellulose β-CD (Kleptose (R)), polysorbate 80 (Tween 80 (TM)) or hyaluronic acid or hyaluronate. The cyclodextrins may also exhibit particularly permeation enhancing properties.
スクアラミンの医薬上許容し得る塩は、酸付加塩、例えば酢酸塩、アジピン酸塩、安息香酸塩、ベンゼンスルホン酸塩、クエン酸塩、樟脳酸塩、デカン酸塩、ドデシル硫酸塩、ヘプタン酸塩、塩酸塩、臭化水素酸塩、乳酸塩、マレイン酸塩、メタンスルホン酸塩、硝酸塩、オレイン酸塩、シュウ酸塩、パルミチン酸塩、リン酸塩、ピバル酸塩、プロピオン酸塩、コハク酸塩、硫酸塩、酒石酸塩、トルエン-p-スルホネート;およびウンデカン酸;および塩基性塩、例えばアンモニウム塩、アルカリ金属塩、例えばナトリウムおよびカリウム塩、アルカリ土類金属塩、例えばカルシウムおよびマグネシウム塩、有機塩基との塩、例えばジシクロヘキシルアミン塩およびアミノ酸、例えばアルギニンとの塩を含むが、これらに限定されない。 Pharmaceutically acceptable salts of squalamine include acid addition salts such as acetate, adipate, benzoate, benzenesulfonate, citrate, camphorate, decanoate, dodecyl sulfate, heptanoate , Hydrochloride, hydrobromide, lactate, maleate, methanesulfonate, nitrate, oleate, oxalate, palmitate, phosphate, pivalate, propionate, succinic acid Salts, sulfate, tartrate, toluene-p-sulfonate; and undecanoic acid; and basic salts such as ammonium salts, alkali metal salts such as sodium and potassium salts, alkaline earth metal salts such as calcium and magnesium salts, organic Including, but not limited to, salts with bases such as dicyclohexylamine salts and salts with amino acids such as arginine.
スクアラミンのモノおよびジ塩双方は、本発明の製剤にとって好適な塩として含まれることが意図される。一例として、スクアラミンのモノラクテートおよびジラクテート塩の双方が含まれる。 Both mono- and di-salts of squalamine are intended to be included as suitable salts for the formulations of the present invention. One example includes both mono- and dilactate salts of squalamine.
特定の実施形態において、該塩はジラクテート塩である。スクアラミンのジラクテート塩は、非晶質形態または結晶形態にて存在する。発明の例示的実施形態において、ジラクテート塩の結晶形態は、溶媒和物として存在する。別の例示的な実施形態において、該結晶形態は、水和物として存在しており、別の実施形態において、ジラクテート塩は溶媒和物および水和物として存在する。スクアラミンジラクテートの結晶形態は、溶媒分子が結晶構造内に組み込まれる場合には、溶媒和物として存在しても良い。例として、該溶媒がエタノールを含有する場合、該結晶はエタノール分子を含有し得る。別の実施形態において、該溶媒和物は水を含有してもよく、該結晶は結晶構造中に水を含有する水和物であってもよい。別の実施形態において、該結晶は、溶媒和物および水和物の双方であってもよい。スクアラミンジラクテートの様々な結晶形態についての記述は、米国特許第7,981,876に見いだされ、この全てを出典明示により本明細書に組み込まれる。 In certain embodiments, the salt is a dilactate salt. The squalamine dilactate salt exists in an amorphous or crystalline form. In an exemplary embodiment of the invention, the crystalline form of the dilactate salt exists as a solvate. In another exemplary embodiment, the crystalline form exists as a hydrate, and in another embodiment, the dilactate salt exists as a solvate and hydrate. The crystalline form of squalamine dilactate may exist as a solvate when solvent molecules are incorporated into the crystal structure. By way of example, if the solvent contains ethanol, the crystals can contain ethanol molecules. In another embodiment, the solvate may contain water and the crystal may be a hydrate containing water in the crystal structure. In another embodiment, the crystals may be both solvates and hydrates. A description of the various crystalline forms of squalamine dilactate is found in US Pat. No. 7,981,876, all of which is incorporated herein by reference.
本明細書に記述した眼用組成物に有用であり得る当業者には既知の典型的な担体、安定化剤およびアジュバントの例示としては、Gennaro (2005) Remington:The Science and Practice of Pharmacy, Mack Publishing、21sted を参照されたい。 Examples of typical carriers, stabilizers and adjuvants known to those skilled in the art that may be useful in the ophthalmic compositions described herein include Gennaro (2005) Remington: The Science and Practice of Pharmacy, Mack. See Publishing, 21 st ed.
本発明のスクアラミン含有組成物のインビボ投与は、単回用量、多回用量にて、処置期間中に連続的また断続的に実行できる。投与の最も有効な用量を決定する方法は、当業者によく知られており、治療に使用される組成物、治療目的および処置される対象によって変化する。単回または多回投与は、治療にあたる医師により選択された用量レベルおよび種類に従って実施できる。 In vivo administration of the squalamine-containing compositions of the present invention can be performed continuously or intermittently during the treatment period, in single or multiple doses. Methods of determining the most effective dosage for administration are well known to those of skill in the art and will vary with the composition used for therapy, the therapeutic purpose and the subject being treated. Single or multiple administrations can be carried out according to the dose level and type selected by the treating physician.
特定の実施形態において、溶液のpHは約7.0〜約7.5の範囲内である。例示的な実施形態において、該溶液は、好ましくは低張溶液である。特定の実施形態において、pHは約7.2〜約7.4である。 In certain embodiments, the pH of the solution is in the range of about 7.0 to about 7.5. In an exemplary embodiment, the solution is preferably a hypotonic solution. In certain embodiments, the pH is about 7.2 to about 7.4.
様々な例示的な実施形態において、本発明の局所製剤は、軟膏、ゲル、クリームまたは点眼薬を含むが、これらに限定されるものではない。 In various exemplary embodiments, the topical formulations of the present invention include, but are not limited to, ointments, gels, creams or eye drops.
様々な特定および非限定製剤を以下に挙げる:
スクアラミンジラクテート+n-ドデシル-β-D-マルトシド+ポビドンK-30+リン酸塩緩衝液;
スクアラミンジラクテート+n-ドデシル-β-D-マルトシド+2-ヒドロキシプロピル-β-シクロデキストリン+ポビドンK-30+リン酸塩緩衝液;
スクアラミンジラクテート+n-ドデシル-β-D-マルトシド+カルボポール980+ホウ酸塩緩衝液;
スクアラミンジラクテート+n-ドデシル-β-D-マルトシド+カルボポール980+リン酸塩緩衝液。
様々な特定の製剤および非限定製剤を下記実施例に記述する。これらの製剤は、本発明の単なる説明であって、本発明の範囲を制限することを意図するものではない。
Various specific and non-limiting formulations are listed below:
Squalamine dilactate + n-dodecyl-β-D-maltoside + povidone K-30 + phosphate buffer;
Squalamine dilactate + n-dodecyl-β-D-maltoside + 2 -hydroxypropyl-β-cyclodextrin + povidone K-30 + phosphate buffer;
Squalamine dilactate + n-dodecyl-β-D-maltoside + carbopol 980 + borate buffer;
Squalamine dilactate + n-dodecyl-β-D-maltoside + carbopol 980 + phosphate buffer.
Various specific and non-limiting formulations are described in the examples below. These formulations are merely illustrative of the invention and are not intended to limit the scope of the invention.
実施例1
製剤A
この製剤は、有効成分として0.2%スクアラミンジラクテート、緩衝液として67 mM NaH2PO4+Na2HPO4(0.9%)、張度改変剤としてNaCl(〜0.4%)、キレート剤/安定化剤としてエデト酸ジナトリウム(0.01%)、防腐剤として塩化ベンザルコニウム(0.005%)および十分量の注射用の水または精製水USPを含む。
Example 1
Formulation A
This formulation consists of 0.2% squalamine dilactate as active ingredient, 67 mM NaH 2 PO 4 + Na 2 HPO 4 (0.9%) as buffer, NaCl (˜0.4%) as tonicity modifier, Contains disodium edetate (0.01%) as a chelator / stabilizer, benzalkonium chloride (0.005%) as a preservative and a sufficient amount of water for injection or purified USP.
製剤Aを次のとおり調製した:50 mLの精製水を、攪拌バーと共に250 mLの目盛り付きガラスビーカーに入れた;2.688 gのリン酸ナトリウム六水和物を、ビーカーに添加して、それが溶解するまで攪拌した;1.24 gのリン酸二水素ナトリウム一水和物を、ビーカーに添加して、それが溶解するまで攪拌した;0.400 gの塩化ナトリウムを、ビーカーに添加して、それが溶解するまで攪拌した;0.005 gの塩化ベンザルコニウムを、ビーカーに添加して、それが溶解するまで攪拌した;0.01 gのEDTA二ナトリウム塩を、ビーカーに添加して、それが溶解するまで攪拌した;0.200 gのスクアラミンジラクテートを、ビーカーに添加して、それが溶解するまで攪拌した;約40 mLの精製滅菌水を、ビーカーに添加した;2N NaOHおよび1N HCl(必要な場合には)を用いて、pHを7.2に調整した;該容量は、十分な量の注射用の水または精製水USPであった。 Formulation A was prepared as follows: 50 mL of purified water was placed in a 250 mL graduated glass beaker with a stir bar; 2.688 g of sodium phosphate hexahydrate was added to the beaker, Stirred until it dissolved; 1.24 g sodium dihydrogen phosphate monohydrate was added to the beaker and stirred until it dissolved; 0.400 g sodium chloride was added to the beaker And stirred until it dissolved; 0.005 g of benzalkonium chloride was added to the beaker and stirred until it dissolved; 0.01 g of EDTA disodium salt was added to the beaker Was stirred until it dissolved; 0.200 g of squalamine dilactate was added to the beaker and stirred until it dissolved; about 40 mL of purified sterile water was added to the beaker. ; 2N NaOH and 1N HCl (if necessary) was used to adjust the pH to 7.2; container weight was water or purified water USP for a sufficient amount of injection.
実施例2
製剤B
この製剤は、有効成分として0.2%スクアラミンジラクテート、緩衝液として67 mM NaH2PO4+Na2HPO4(0.9%)、張度改変剤としてNaCl(〜0.4%)、キレート剤/安定化剤としてエデト酸二ナトリウム塩(0.01%)、粘膜接着剤としてカルボポール980NF(0.5%)および十分な量の注射用の水または精製水USPを含む。
Example 2
Formulation B
This formulation consists of 0.2% squalamine dilactate as active ingredient, 67 mM NaH 2 PO 4 + Na 2 HPO 4 (0.9%) as buffer, NaCl (˜0.4%) as tonicity modifier, Edetate disodium salt (0.01%) as chelating agent / stabilizer, carbopol 980NF (0.5%) as mucoadhesive agent and a sufficient amount of water for injection or purified water USP.
製剤Bを次のとおり調製した:50 mLの精製水を、250 mLの攪拌バーと共に250 mLの目盛り付きガラスビーカーに入れた;2.688 gのリン酸ナトリウム六水和物を、ビーカーに添加して、それが溶解するまで攪拌した;1.24 gのリン酸二水素ナトリウム一水和物を、ビーカーに添加して、それが溶解するまで攪拌した;0.400 gの塩化ナトリウムを、ビーカーに添加して、それが溶解するまで攪拌した;0.01 gのEDTA二ナトリウムを、ビーカーに添加して、それが溶解するまで攪拌した;0.200 gのスクアラミンジラクテートを、ビーカーに添加して、それが溶解するまで攪拌した;0.500 gのカルボポール980NFを、ビーカーに添加して、それが溶解するまで攪拌した;約40 mLの精製滅菌水を、ビーカーに添加した;該pHを、2N NaOHおよび1N HCl(必要な場合には)を用いて7.2に調整した;該容量を、100 mLまでとした;そして、該溶液を、0.22ミクロンフィルターを有する滅菌濾過アセンブリを用いて濾過した。 Formulation B was prepared as follows: 50 mL of purified water was placed in a 250 mL graduated glass beaker with a 250 mL stirring bar; 2.688 g of sodium phosphate hexahydrate was added to the beaker. And stirred until it dissolved; 1.24 g of sodium dihydrogen phosphate monohydrate was added to the beaker and stirred until it dissolved; 0.400 g of sodium chloride Added to beaker and stirred until it dissolved; 0.01 g EDTA disodium was added to the beaker and stirred until it dissolved; 0.200 g squalamine dilactate was added to the beaker. And stirred until it dissolved; 0.500 g Carbopol 980NF was added to the beaker and stirred until it dissolved; about 40 mL of purified sterile water was added to The pH was adjusted to 7.2 with 2N NaOH and 1N HCl (if necessary); the volume was brought up to 100 mL; and the solution was 0.22 Filter using a sterile filtration assembly with a micron filter.
実施例3
製剤C
この製剤は、有効成分として0.2%スクアラミンジラクテート、緩衝液として67 mM NaH2PO4+Na2HPO4(0.9%)、張度改変剤としてマンニトール(〜0.8%)、キレート剤/安定化剤としてエデト酸ジナトリウム(0.01%)、粘膜接着剤としてカルボポール980NF(0.5%)、浸透増強剤としてn-ドデシル-β-D-マルトシド(0.05-0.1%)、防腐剤として塩化ベンザルコニウム(0.005%)および十分な量の注射用の水または精製水USPを含む。
Example 3
Formulation C
This formulation consists of 0.2% squalamine dilactate as the active ingredient, 67 mM NaH 2 PO 4 + Na 2 HPO 4 (0.9%) as a buffer, mannitol (˜0.8%) as a tonicity modifying agent, Edetate disodium (0.01%) as chelating agent / stabilizer, Carbopol 980NF (0.5%) as mucoadhesive agent, n-dodecyl-β-D-maltoside (0.05- 0.1%), benzalkonium chloride (0.005%) as a preservative and a sufficient amount of water for injection or purified water USP.
製剤Cを次のとおり調製した:50 mLの精製水を、攪拌バーと共に250 mLの目盛り付きガラスビーカーに入れた;2.688 g のリン酸ナトリウム六水和物を、ビーカーに添加して、それが溶解するまで攪拌した;1.24 gのリン酸二水素ナトリウム一水和物を、ビーカーに添加して、それが溶解するまで攪拌した;0.800 gのマンニトールを、ビーカーに添加して、それが溶解するまで攪拌した;0.005 gの塩化ベンザルコニウムを、ビーカーに添加して、それが溶解するまで攪拌した;0.01 gのEDTA二ナトリウムを、ビーカーに添加して、それが溶解するまで攪拌した;0.500 gのカルボポール980NFを、ビーカーに添加して、それが溶解するまで攪拌した;0.200 gのスクアラミンジラクテートを、ビーカーに添加して、それが溶解するまで攪拌した;0.05 gのn-ドデシル-β-D-マルトシドを、ビーカーに添加して、それが溶解するまで攪拌した;約40 mLの精製滅菌水を、ビーカーに添加した;該pHを、2N NaOHおよび1N HCl(必要な場合には)を用いて7.2に調整した;該容量を、100 mLまでとした;そして、該溶液を、0.22ミクロンフィルターを有する滅菌濾過アセンブリを用いて濾過した。 Formulation C was prepared as follows: 50 mL of purified water was placed in a 250 mL graduated glass beaker with a stir bar; 2.688 g of sodium phosphate hexahydrate was added to the beaker; Stirred until it dissolved; 1.24 g sodium dihydrogen phosphate monohydrate was added to the beaker and stirred until it dissolved; 0.800 g mannitol was added to the beaker. Stirred until it dissolved; 0.005 g benzalkonium chloride was added to the beaker and stirred until it dissolved; 0.01 g disodium EDTA was added to the beaker. Stirred until it dissolved; 0.500 g carbopol 980NF was added to the beaker and stirred until it dissolved; 0.200 g squalamine dilactate was added to the beaker. Added and stirred until it dissolved; 0.05 g n-dodecyl-β-D-maltoside was added to the beaker and stirred until it dissolved; about 40 mL of purified sterile water was added. The pH was adjusted to 7.2 using 2N NaOH and 1N HCl (if needed); the volume was brought up to 100 mL; Filtration using a sterile filtration assembly with a 22 micron filter.
実施例4
製剤D
この製剤は、有効成分として0.1%スクアラミンジラクテート、緩衝液として50 mM NaH2PO4+Na2HPO4(0.9%)、張度改変剤としてNaCl(〜0.9%)、キレート剤/安定化剤としてエデト酸ジナトリウム(0.01%)、粘膜接着剤としてヒドロキシプロピル-メチルセルロース、防腐剤として塩化ベンザルコニウム(0.005%)および十分な量の注射用の水または精製水USPを含む。この製剤を、上記製剤と同様の方法にて製造した。
Example 4
Formulation D
This formulation consists of 0.1% squalamine dilactate as active ingredient, 50 mM NaH 2 PO 4 + Na 2 HPO 4 (0.9%) as buffer, NaCl (˜0.9%) as tonicity modifier, Edetate disodium (0.01%) as a chelating agent / stabilizer, hydroxypropyl-methylcellulose as a mucoadhesive agent, benzalkonium chloride (0.005%) as a preservative and a sufficient amount of water for injection or Contains purified water USP. This preparation was produced in the same manner as the above preparation.
実施例5
製剤E
この製剤は、有効成分として0.2%スクアラミンジラクテート、緩衝液として67 mM NaH2PO4+Na2HPO4(0.9%)、張度改変剤としてNaCl(〜0.4%)、キレート剤/安定化剤としてエデト酸ジナトリウム(0.01%)、粘膜接着剤としてヒドロキシプロピル-メチルセルロースおよび十分な量の注射用の水または精製水USPを含む。
Example 5
Formulation E
This formulation consists of 0.2% squalamine dilactate as active ingredient, 67 mM NaH 2 PO 4 + Na 2 HPO 4 (0.9%) as buffer, NaCl (˜0.4%) as tonicity modifier, Contains disodium edetate (0.01%) as a chelating agent / stabilizer, hydroxypropyl-methylcellulose as a mucoadhesive agent and a sufficient amount of water for injection or purified USP.
この製剤を、上記製剤と同様の方法にて製造した。 This preparation was produced in the same manner as the above preparation.
実施例6
製剤F
この製剤は、有効成分として0.1%スクアラミンジラクテート、緩衝液としてホウ酸(0.8%)+ホウ酸ナトリウム(0.12%)、張度改変剤としてマンニトール(〜0.8%)、キレート剤/安定化剤としてαトコフェロール(0.005%)、粘膜接着剤としてカルボポール980NF(0.5%)、浸透増強剤としてn-ドデシル-β-D-マルトシド(0.05−0.1%)、防腐剤として塩化ベンザルコニウム(0.005%)および十分な量の注射用の水または精製水USPを含む。
Example 6
Formulation F
This formulation contains 0.1% squalamine dilactate as the active ingredient, boric acid (0.8%) + sodium borate (0.12%) as the buffer, and mannitol (˜0.8% as the tonicity modifier). ), Α-tocopherol (0.005%) as chelating agent / stabilizer, carbopol 980NF (0.5%) as mucoadhesive agent, n-dodecyl-β-D-maltoside (0.05-) as penetration enhancer 0.1%), benzalkonium chloride (0.005%) as a preservative and a sufficient amount of water for injection or purified water USP.
この製剤を、上記製剤と同様の方法にて製造した。 This preparation was produced in the same manner as the above preparation.
実施例7
製剤G
この製剤は、有効成分として0.2%スクアラミンジラクテート、緩衝液としてリン酸ナトリウム六水和物1.88% w/vおよびリン酸二水素ナトリウム一水和物1.0% w/v、皮膚軟化剤としてポビドンK-30 1.2% w/v、安定化剤としてエデト酸二ナトリウム0.01%、浸透増強剤としてn-ドデシル-β-D-マルトシド0.005% w/v、防腐剤として塩化ベンザルコニウム0.005% w/v、可溶化剤として2-ヒドロキシプロピル-β‐シクロデキストリン0.9% w/vおよび精製水qsを含む。pH=6.70およびオスモル濃度=315 mOsm/kg。該溶液を、使用前に0.22ミクロンフィルターを通して滅菌濾過した。
Example 7
Formulation G
This formulation contains 0.2% squalamine dilactate as the active ingredient, sodium phosphate hexahydrate 1.88% w / v as buffer and sodium dihydrogen phosphate monohydrate 1.0% w / v. Povidone K-30 1.2% w / v as emollient, disodium edetate 0.01% as stabilizer, n-dodecyl-β-D-maltoside 0.005% w / v as penetration enhancer Benzalkonium chloride 0.005% w / v as preservative, 2 -hydroxypropyl-β-cyclodextrin 0.9% w / v as solubilizer and purified water qs. pH = 6.70 and osmolality = 315 mOsm / kg. The solution was sterile filtered through a 0.22 micron filter before use.
この製剤を、上記製剤と同様の方法にて製造した。 This preparation was produced in the same manner as the above preparation.
実施例8
製剤H
この製剤は、有効成分として0.2%スクアラミンジラクテート、皮膚軟化剤としてグリセリン1% w/v、緩衝液としてホウ酸1.18% w/vおよびホウ酸ナトリウム0.12% w/v、浸透増強剤としてn-ドデシル-β-D-マルトシド0.005% w/v、防腐剤として塩化ベンザルコニウム0.005%および精製水qsを含む。pH=6.90およびオスモル濃度=305 mOsm/kg。該溶液を、使用前に0.22ミクロンフィルターを通して滅菌濾過した。
Example 8
Formulation H
This formulation contains 0.2% squalamine dilactate as the active ingredient,
この製剤を、上記製剤と同様の方法にて製造した。 This preparation was produced in the same manner as the above preparation.
実施例9
製剤I
この製剤は、有効成分として0.2%スクアラミンジラクテート、緩衝液としてリン酸ナトリウム塩六水和物1.88% w/vおよびリン酸二水素ナトリウム塩一水和物0.87% w/v、張度改変剤として塩化ナトリウム0.3 % w/v、安定化剤としてエデト酸二ナトリウム0.01%、防腐剤として塩化ベンザルコニウム0.005% w/v、可溶化剤として2-ヒドロキシプロピル-β-シクロデキストリン0.9% w/vおよび精製水qsを含有した。pH= 6.72およびオスモル濃度=325 mOsm/kg。該溶液を、使用前に0.22ミクロンフィルターを通して滅菌濾過した。
Example 9
Formulation I
This formulation contains 0.2% squalamine dilactate as the active ingredient, 1.88% w / v sodium phosphate hexahydrate as buffer and 0.87% w sodium dihydrogen phosphate monohydrate. / v, sodium chloride 0.3% w / v as tonicity modifier, disodium edetate 0.01% as stabilizer, benzalkonium chloride 0.005% w / v as preservative, solubilizer It contained 2 -hydroxypropyl- β -cyclodextrin 0.9% w / v and purified water qs. pH = 6.72 and osmolality = 325 mOsm / kg. The solution was sterile filtered through a 0.22 micron filter before use.
この製剤を、上記製剤と同様の方法にて製造した。 This preparation was produced in the same manner as the above preparation.
実施例10
製剤J
この製剤は、有効成分として0.2%スクアラミンジラクテート、緩衝液としてリン酸ナトリウム塩六水和物1.88% w/vおよびリン酸二水素ナトリウム塩一水和物1.0% w/v、皮膚軟化剤としてポピドンK-30 0.6% w/v、安定化剤としてエデト酸二ナトリウム0.01%、浸透増強剤としてn-ドデシル-β-D-マルトシド0.005% w/v、防腐剤として塩化ベンザルコニウム0.005% w/vおよび精製水qsを含む。pH=6.70およびオスモル濃度=295 mOsm/kg。該溶液を、使用前に0.22ミクロンフィルターを通して滅菌濾過した。
Example 10
Formulation J
This formulation contains 0.2% squalamine dilactate as the active ingredient, sodium phosphate hexahydrate 1.88% w / v as buffer and sodium dihydrogen phosphate monohydrate 1.0% w / v, Popidone K-30 0.6% w / v as emollient, Disodium edetate 0.01% as stabilizer, n-dodecyl-β-D-maltoside 0.005% w as penetration enhancer / v, containing benzalkonium chloride 0.005% w / v as preservative and purified water qs. pH = 6.70 and osmolality = 295 mOsm / kg. The solution was sterile filtered through a 0.22 micron filter before use.
この製剤を、上記製剤と同様の方法にて製造した。 This preparation was produced in the same manner as the above preparation.
実施例11
製剤K
この製剤は、有効成分として0.2%スクアラミンジラクテート、皮膚軟化剤としてグリセリン1.0% w/v、張度改変剤としてマンニトール0.05% w/v、緩衝液としてホウ酸1.18 % w/vおよびホウ酸ナトリウム0.12% w/v、張度改変剤として塩化ナトリウム0.4% w/v、浸透増強剤としてn-ドデシル-β-D-マルトシド0.005% w/v、防腐剤として塩化ベンザルコニウム0.005% w/vおよび精製水qsを含む。pH=5.86およびオスモル濃度=285 mOsm/kg。該溶液を、使用前に0.22ミクロンフィルターを通して滅菌濾過した。
Example 11
Formulation K
This formulation contains 0.2% squalamine dilactate as an active ingredient, glycerin 1.0% w / v as an emollient, mannitol 0.05% w / v as a tonicity modifier, and
この製剤を、上記製剤と同様の方法にて製造した。 This preparation was produced in the same manner as the above preparation.
実施例12
スクアラミンラクテート製剤に対する安定性試験
製剤GおよびH(上記を参照されたい)を、2週間、1ヶ月、3ヶ月、および6ヶ月間、室温および40℃での安定性について試験した。スクアラミンラクテート濃度を、各時点でHPLCにより評価し(表1)、該製剤の安定性を肉眼観察およびpHにより評価した(表2)。スクアラミンラクテートおよび該製剤は、全ての時点で安定であることが判った。
Example 12
Stability Tests for Squalamine Lactate Formulations Formulations G and H (see above) were tested for stability at room temperature and 40 ° C. for 2 weeks, 1 month, 3 months, and 6 months. Squalamine lactate concentration was assessed by HPLC at each time point (Table 1), and the stability of the formulation was assessed by visual observation and pH (Table 2). Squalamine lactate and the formulation were found to be stable at all time points.
表1:
表2:
スクアラミンラクテート製剤の安定性
Stability of squalamine lactate formulations
実施例13
ウサギの眼への局所投与によるスクアラミンラクテート製剤の耐性試験
スクアラミンラクテート製剤Gおよびスクアラミンラクテート製剤H(上記製剤を参照されたい)を、ダッチベルテッド種ウサギに、局所点眼により1日1回として28日間投与した場合の眼の滞留について評価した。ビヒクルコントロールは、スクアラミンラクテートを含まないスクアラミンラクテート製剤であった。
Example 13
Tolerance test of squalamine lactate formulation by topical administration to the rabbit eye Squalamine lactate formulation G and squalamine lactate formulation H (see above formulation) were applied to Dutch belted rabbits once daily by topical instillation. The retention of the eye when administered for 28 days was evaluated. The vehicle control was a squalamine lactate formulation without squalamine lactate.
試験計画は以下のとおりであった:
以下のパラメーターおよびエンドポイントをこの試験で評価した:臨床徴候、体重、体重変化、眼科学、眼球内圧、肉眼的眼試験、肉眼的剖検所見および組織学的試験。死亡は観察されず、体重および体重増加に対して処置と関連した効果はなかった。また、処置に関連した眼科的所見、眼球内圧に対する影響もなく、肉眼または顕微鏡的所見もなかった。これらの所見に基づいて、該製剤は安全であり、眼の毒性に関する徴候はなかった。 The following parameters and endpoints were evaluated in this study: clinical signs, body weight, weight change, ophthalmology, intraocular pressure, gross eye test, gross autopsy findings and histological examination. No death was observed and there was no treatment-related effect on body weight and weight gain. There were also no ophthalmic findings related to treatment, no effect on intraocular pressure, and no gross or microscopic findings. Based on these findings, the formulation was safe and there were no signs of ocular toxicity.
処置と関連した眼の充血および/または分泌(discharge)および稀な膨潤が、>38.4 μg/kg/日のスクアラミンラクテート製剤Gおよび/または>39μg/kg/日のスクアラミンラクテート製剤Hおよび/またはビヒクルコントロールBを与えた動物の眼(両眼含む)で見られ、スクアラミンラクテート製剤Hを投与した動物では一般的に増大した事象を伴う。透明な分泌物の軽度の臨床徴候と相関した分泌物の所見は、両方のスクアラミンラクテート製剤を投与した動物およびビヒクルコントロールBを投与した動物において14日目に見られた。これらの所見から、その低い重症度(一般的には、正常からの非常に僅かまたは幾らかの逸脱)および眼科的、肉眼的または顕微鏡的相関性の欠如が示され、副作用がないと考察した。 Ocular engorgement and / or discharge and rare swelling associated with the treatment may result in > 38.4 μg / kg / day squalamine lactate formulation G and / or > 39 μg / kg / day squalamine lactate formulation H And / or is seen in the eyes (including both eyes) of animals given vehicle control B and is generally associated with increased events in animals administered squalamine lactate formulation H. Secretory findings correlated with mild clinical signs of clear secretions were seen on day 14 in animals receiving both squalamine lactate formulations and animals receiving vehicle control B. These findings indicate their low severity (generally very little or some deviation from normal) and lack of ophthalmic, macroscopic or microscopic correlation and no side effects .
結論として、1日1回の局所点眼による0、38.4、57.6および96μg/kg/日でのスクアラミンラクテート製剤Gの投与および0、39、58.5および97.5μg/kg/日でのスクアラミンラクテート製剤Hの投与は、一般的にダッチベルテッド種ウサギにおいて十分耐性であった。これらの結果に基づいて、観察されない副作用レベル(NOAEL)は、96μg/kg/日(スクアラミンラクテート製剤G)または97.5μg/kg/日(スクアラミンラクテート製剤H)であると考えられ、スクアラミンラクテート製剤Hの全ての用量および時折ビヒクルコントロールBを投与した動物における充血および分泌物に関する僅かな眼の知見に基づくと、スクアラミンラクテート製剤GおよびビヒクルコントロールAは、スクアラミンラクテート製剤HおよびビヒクルコントロールBよりも、より耐性が高いと考えられる。 In conclusion, administration of squalamine lactate formulation G at 0, 38.4, 57.6 and 96 μg / kg / day by topical instillation once daily and 0, 39, 58.5 and 97.5 μg / kg / day Administration of squalamine lactate formulation H on a daily basis was generally well tolerated in Dutch-belted rabbits. Based on these results, the unobserved side effect level (NOAEL) is considered to be 96 μg / kg / day (squalamine lactate formulation G) or 97.5 μg / kg / day (squalamine lactate formulation H), Based on slight eye knowledge of hyperemia and secretion in animals dosed with all doses of lamin lactate formulation H and occasionally vehicle control B, squalamine lactate formulation G and vehicle control A were treated with squalamine lactate formulation H and vehicle. It is considered that the tolerance is higher than that of the control B.
実施例14
眼投与後のダッチベルテッド種ウサギにおけるスクアラミンラクテート製剤の眼の生体内分布試験
Example 14
Ocular biodistribution study of squalamine lactate preparations in Dutch-belted rabbits after ocular administration
本試験の目的は、雄ダッチベルテッド種ウサギへの眼投与により1回投与した場合の、スクアラミンラクテート製剤G(上記組成物を参照されたい)の眼の生体内分布を決定することであった。 The purpose of this study was to determine the ocular biodistribution of squalamine lactate formulation G (see above composition) when administered once by ocular administration to male Dutch belted rabbits. .
試験計画は下記のとおりである:
試験計画
Test plan
体重測定値を、無作為化/用量の算定目的のために取得した。処置と関連する臨床徴候は、眼投与後に観察されなかった。用量投与後に、血液試料を、特定の時点で採取して、血漿を調製した。血液試料の採取後に、動物を安楽死させて、剖検を行い、以下の眼組織を回収した:房水、硝子体液、感覚網膜および脈絡膜/強膜。血漿および眼の組織を分析して、これらの分析結果を下記表に示した。
スクアラミンの定量可能なレベルは、いずれの動物の房水または硝子体液中でも検出されず、スクアラミンが、角膜の全ての層を有意に透過しないか、あるいはレンズと接触しないことを確認した。結論として、スクアラミンラクテート量についての眼組織の分析結果は、3時間の時点でさえ、後部強膜および脈絡膜中でHUVAC血管形成を妨害するのに十分なレベルを示す(以下の図1および実施例15を参照されたい)。それ故に、これらのレベルが、ウェット型AMDにて起こる有害な脈絡膜血管新生(CNV)過程を阻止するのに十分であることが推定される(例えば、Invest. Ophthalmol. Vis. Sci. February 2005 vol. 46 no. 2 454-460 and US patent application publication # 2010/0272719を参照されたい)。 No quantifiable level of squalamine was detected in the aqueous humor or vitreous humor of any animal, confirming that squalamine does not significantly penetrate all layers of the cornea or contact the lens. In conclusion, ocular tissue analysis results for squalamine lactate levels show sufficient levels to interfere with HUVAC angiogenesis in the posterior sclera and choroid, even at 3 hours (see Figure 1 and below). See Example 15). It is therefore presumed that these levels are sufficient to prevent the deleterious choroidal neovascularization (CNV) process that occurs in wet AMD (eg, Invest. Ophthalmol. Vis. Sci. February 2005 vol. 46 no. 2 454-460 and US patent application publication # 2010/0272719).
実施例15
スクアラミンを用いるHUVECによるVEGF誘導性血管形成の阻害
スクアラミンラクテートを、50、100または200nM濃度の溶液中でヒト血管内皮細胞(HUVEC)の懸濁液と共に混合した。次いで、該懸濁液を、直ぐに血管内皮細胞成長因子(VEGF)を含む複数の成長因子を含有したMatrigel上に播種した。該プレートを、24時間95%O2/5%CO2の大気中において37℃でインキュベートし、次いでプレートを撮影した。結果を図1に示し、スクアラミンが50nM濃度でさえ血管形成を妨害することを示す。
Example 15
Inhibition of VEGF-induced angiogenesis by HUVEC using squalamine Squalamine lactate was mixed with a suspension of human vascular endothelial cells (HUVEC) in a solution of 50, 100 or 200 nM concentration. The suspension was then immediately seeded on Matrigel containing multiple growth factors including vascular endothelial growth factor (VEGF). The plates were incubated for 24 hours in an atmosphere of 95% O 2 /5% CO 2 at 37 ° C., then the plates were photographed. The results are shown in FIG. 1 and show that squalamine interferes with angiogenesis even at a concentration of 50 nM.
多くの文献を引用するが、この全ての開示内容を出典明示により本明細書に組み込む。 Many references are cited, the entire disclosure of which is incorporated herein by reference.
Claims (15)
ジラクテート塩としてのスクアラミン;
ポビドンK-30;
ヒドロキシプロピル-β-シクロデキストリン;
リン酸緩衝剤;および
水
を含んでおり、
治療上有効量にて予防または処置が必要な哺乳動物の眼に投与され、前記スクアラミンを哺乳動物の眼の後部強膜および脈絡膜に選択的に送達する、医薬組成物。 A pharmaceutical composition for preventing or treating ocular symptoms in a mammal, comprising:
Sukuarami down as dilactate salt;
Povidone K-30;
Hydroxypropyl-β-cyclodextrin;
A phosphate buffer; and
Water <br/>
A pharmaceutical composition, which is administered to a mammal eye in need of prevention or treatment in a therapeutically effective amount and selectively delivers the squalamine to the posterior sclera and choroid of the mammal eye .
ジラクテート塩としてのスクアラミン;
ポビドンK-30;
ヒドロキシプロピル-β-シクロデキストリン;
リン酸緩衝剤;および
水
を含み、房水または硝子体液中には無視できる濃度の前記スクアラミンをもたらす、医薬組成物。 A pharmaceutical composition for selectively delivering in a therapeutically effective amount of squalamine selectively to the posterior sclera and choroid of a mammalian eye in need thereof,
Squalamine as dilactate salt;
Povidone K-30;
Hydroxypropyl-β-cyclodextrin;
A phosphate buffer; and
water
A pharmaceutical composition comprising a negligible concentration of said squalamine in aqueous humor or vitreous humor .
ポビドンK-30;
ヒドロキシプロピル-β-シクロデキストリン;
リン酸緩衝剤;および
水
を含む、眼用組成物。 Sukuarami down as dilactate salt;
Povidone K-30;
Hydroxypropyl-β-cyclodextrin;
A phosphate buffer; and
An ophthalmic composition comprising water .
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| Application Number | Priority Date | Filing Date | Title |
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| US37452410P | 2010-08-17 | 2010-08-17 | |
| US61/374,524 | 2010-08-17 | ||
| PCT/US2011/047920 WO2012024298A1 (en) | 2010-08-17 | 2011-08-16 | Ophthalmic formulations of squalamine |
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| RU2768652C1 (en) * | 2014-09-17 | 2022-03-24 | Паноптика, Инк. | Ophthalmic formulations for drug delivery and anterior eye protection |
| WO2017083799A1 (en) * | 2015-11-13 | 2017-05-18 | Ohr Pharmaceutical, Inc. | Ophthalmic formulations of squalamine |
| TW201720446A (en) * | 2015-11-13 | 2017-06-16 | Ohr製藥公司 | Occult CNV size as a predictor for treatment with squalamine |
| KR20180036580A (en) | 2016-09-30 | 2018-04-09 | 주식회사 유스바이오팜 | Composition for prevention or treatment of inflammatory skin diseases or severe pruritus comprising the aqueous solubilized ursodeoxycholic acid |
| WO2018185788A1 (en) * | 2017-04-07 | 2018-10-11 | Sun Pharma Advanced Research Company Limited | Ophthalmic solution of bimatoprost |
| IT202300017430A1 (en) * | 2023-08-22 | 2025-02-22 | Service Biotech srl | OPHTHALMIC SOLUTION IN THE FORM OF EYE DROPS CONTAINING A RECOMBINANT HUMAN ISOFORM OF MANGANESE SUPEROXIDE DISMUTASE (RMNSOD) FOR THE TREATMENT OF EYE DISEASES |
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| EP0444778A1 (en) * | 1990-02-14 | 1991-09-04 | Alcon Laboratories, Inc. | Use of alkyl saccharides to enhance the penetration of drugs |
| US5631004A (en) * | 1993-09-30 | 1997-05-20 | Alcon Laboratories, Inc. | Use of sustained release antibiotic compositions in ophthalmic surgical procedures |
| WO1997026888A1 (en) | 1996-01-26 | 1997-07-31 | Alcon Laboratories, Inc. | Use of squalamine and its analogues in ophthalmic compositions |
| US6262283B1 (en) | 1996-12-06 | 2001-07-17 | Magainin Pharmaceuticals Inc. | Stereoselective synthesis of 24-hydroxylated compounds useful for the preparation of aminosterols, vitamin D analogs, and other compounds |
| US20060172972A1 (en) * | 2002-12-20 | 2006-08-03 | Chakshu Research Inc | Formulation and method for administration of ophthalmologically active agents |
| US20050234018A1 (en) * | 2004-04-15 | 2005-10-20 | Allergan, Inc. | Drug delivery to the back of the eye |
| US20080233053A1 (en) * | 2005-02-07 | 2008-09-25 | Pharmalight Inc. | Method and Device for Ophthalmic Administration of Active Pharmaceutical Ingredients |
| ES2732251T3 (en) * | 2005-04-25 | 2019-11-21 | Enterin Inc | Crystalline Squalamine Dilactate |
| WO2006119211A2 (en) * | 2005-05-02 | 2006-11-09 | Genaera Corporation | Methods and compositions for treating ocular disorders |
| AU2006270035A1 (en) * | 2005-07-15 | 2007-01-25 | Chakshu Research Inc. | Formulation and method for administration of ophthalmologically active agents |
| US7893040B2 (en) * | 2005-07-22 | 2011-02-22 | Oculis Ehf | Cyclodextrin nanotechnology for ophthalmic drug delivery |
| AU2006316607A1 (en) * | 2005-11-21 | 2007-05-31 | Schering-Plough Pty. Limited | Pharmaceutical compositions comprising buprenorphine |
| US8216575B2 (en) | 2006-03-31 | 2012-07-10 | Chengdu Kanghong Biotechnologies Co., Ltd. | Inhibition of neovascularization with a soluble chimeric protein comprising VEGF FLT-1 and KDR domains |
| WO2008031113A2 (en) * | 2006-09-08 | 2008-03-13 | Genaera Corporation | Improved method for inhibition of neovascularization |
| GB0625844D0 (en) * | 2006-12-22 | 2007-02-07 | Daniolabs Ltd | The treatment of macular degeneration |
| US8821870B2 (en) | 2008-07-18 | 2014-09-02 | Allergan, Inc. | Method for treating atrophic age related macular degeneration |
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| JP2013537551A (en) | 2013-10-03 |
| AU2011292160B2 (en) | 2015-09-03 |
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| EP2605752A1 (en) | 2013-06-26 |
| CN106074362A (en) | 2016-11-09 |
| JP6214726B2 (en) | 2017-10-18 |
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| AU2011292160A1 (en) | 2013-03-14 |
| US20150342874A1 (en) | 2015-12-03 |
| US20130281420A1 (en) | 2013-10-24 |
| KR101845107B1 (en) | 2018-04-03 |
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| WO2012024298A1 (en) | 2012-02-23 |
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